Objective

Multiple trauma is often accompanied by systemic inflammatory response syndrome (SIRS). The aim of this study was to investigate the impact of polymeric plasma substitutes on the development of SIRS or sepsis.

Methods

We included 2969 patients aged ≥16 years with an Injury Severity Score (ISS) >16 in this study. The sample was subdivided into three groups: patients who did not receive colloids and those who received <5L colloids and >5L colloids within the first 48 h. Data were analyzed using IBM SPSS® for Windows version 22.0; analysis of variance was used for continuous normally distributed data and Kruskal–Wallis test for categorical data. The predictive quality of colloid treatment was analyzed using the receiver operating characteristic (ROC) curves. Independent predictively was analyzed by binary logistic regression. Data were considered significant if P < 0.05. Data are presented as the mean ± standard deviation.

Results

The SIRS score increased with the amount of colloid used (1.9 ± 1.4 vs. 2.4 ± 1.2 vs. 3.2 ± 0.9; P < 0.001). However, the predictive quality was low, with an area under the ROC of 0.693 for SIRS and 0.669 for sepsis (P < 0.001). Binary logistic regression revealed colloids as an independent factor for the development of SIRS and sepsis (odds ratios: SIRS 3.325 and sepsis 8.984; P < 0.001).

Conclusion

Besides other factors, colloids have a significant permissive effect and are independent predictors for the development of SIRS and sepsis in multiply injured patients.

The most frequent cause of death in the young and productive adult population is trauma. Bleeding, surgery, and coagulopathy are the main killers of severely injured patients [1, 2]. The more severely a patient is injured, the more they tend to bleed and develop systemic inflammatory response syndrome (SIRS) [3]. Besides emergency surgical interventions, efficient infusion therapy in severely injured patients is the key method of improving the survival of patients. According to Advanced Trauma Life Support (ATLS) guidelines, the initial volume therapy should be administered in a balanced way with further ongoing saline or transfusion therapy according to the patient’s physiological state with a permissive hypotension. The symptoms of SIRS in severe injury resemble a systemic disease. During the last decade, hydroxyethyl starch derivates (HES) and other colloids have been extensively postulated as therapeutic agents to prevent capillary leakage during SIRS and to influence blood coagulation [4–6]. Overactivation of the immune system during SIRS leads to its depression through the compensatory anti-inflammatory response syndrome (CARS). In this phase, multiply injured patients are highly susceptible to infections, which increase their mortality and hospitalization. Positive immunomodulation by an appropriate infusion therapy in multiply injured patients could be very useful for improving the survival and outcome of these patients. Hospitalization could be shortened, leading to a decrease in treatment costs. The colloids included in this study are both HES and modified gelatin. The absence of clear infusion protocols for colloidal plasma expanders may lead to involuntary mixtures of infused colloids. In this retrospective cohort study, we asked how colloids influence the development of SIRS and sepsis in patients with multiple traumas, apart from other factors with a significant permissive effect on the development of SIRS and sepsis.

Patient sample

In this retrospective cohort study, we included 2969 patients with severe injuries admitted to the trauma bay of the University Hospital of Zürich (Switzerland) during the period 1996–2011. The data from 120 patients were incomplete and excluded from this study. The inclusion criteria were an Injury Severity Score (ISS) >16 points, age ≥16 years, and admission within at least 24 h of incurring the severe injury. The patient sample was subdivided into three groups (Table 1) according to the use or otherwise of colloids. All patient data were collected retrospectively. The observation period was 30 days maximally or until the discharge of the patient. The data were retrieved from patient records with the approval of the local institutional review board (IRB) according to the University of Zürich IRB guidelines and the World Medical Association Declaration of Helsinki. The study was conducted according to our institutional guidelines for good clinical practice (Ethics Committee of the University Hospital of Zürich Permission: ‘Retrospektive Analysen in der Chirurgischen Intensivmedizin’ No. St. V. 01-2008). No individual consent was required. The data were not age or sex matched.

Table 1

The characteristics of the patient sample at admission for those not receiving colloids vs. receiving colloids <5L/48 h vs. colloids >5L/48 h

Diagnostic protocol

Unstable patients underwent resuscitative procedures according to the ATLS guidelines of the American College of Surgeons. Hemodynamically stable patients received diagnoses according to clinical findings or whole-body computed tomography (CT) in uncertain situations. Hemodynamically unstable patients received focus-oriented diagnostics with immediate problem solving according to the ATLS guidelines.

Primary care

The treatment of all patients admitted was according to the ATLS guidelines and the previously assessed trauma management protocol, after appropriate indications had been identified [7, 8].

Scoring systems

The overall physiological impairment was evaluated from the Acute Physiology and Chronic Health Evaluation (APACHE II) score of the patient at admission [9]. The ISS and the New Injury Severity Scale (NISS) were used to define the severity of trauma [10, 11]. The Abbreviated Injury Scale (AIS; 2005 version) was used to describe injuries in specific anatomical regions.

Laboratory parameters

Blood lactate levels, pH, and hematocrits were measured at intervals using a blood gas analyzer (ABL800 Flex, Radiometer, Thalwil, Switzerland). The prothrombin time was measured using a standardized method [12].

Transfusion resuscitation of multiply injured patients

Infusion and transfusion therapies for multiply injured patients were applied according to damage control resuscitation criteria [13] and the guidelines of the University Hospital of Zurich [14].

Assessment of SIRS and sepsis

The worst values for leukocyte count, respiratory rate, heart rate, and temperature were taken to determine the SIRS score each day [15]. SIRS was measured during the first 30 days after admission or as long as the patients were hospitalized. Sepsis was defined as an SIRS score ≥2 with an infectious focus.

Statistical analysis

Data are presented as the mean ± standard deviation for continuous variables and as percentages for categorical variables. Cases with an incomplete data set were discarded from this study (n = 52). Two-tailed Kolmogorov–Smirnov tests were used for testing normality and, if P < 0.05, the data were considered to be normally distributed. The data for the groups were compared using a χ2 test and a Kruskal–Wallis test for categorical data and one-way analysis of variance (ANOVA) for continuous data. If a Kolmogorov–Smirnov test showed P > 0.05, Mann–Whitney non-parametric U test was used for continuous data. Results were considered significant if P < 0.05. The predictive quality for SIRS and sepsis of colloids was reported as the area under the receiver operator characteristic (ROC) curve. The entire amount of infused colloids was used as a predictor for SIRS and sepsis. Odds ratios (ORs) were calculated for categorical data. Independent predictivity was analyzed using binary logistic regression with the Hosmer–Lemeshow test for the goodness of fit; good if P > 0.05. Data were analyzed using IBM SPSS Statistics for Windows software (version 22.0; IBM Corp., Armonk, NY, USA).

Patients not receiving colloids vs. receiving colloids <5L/48h vs. colloids >5L/48h are compared. The sequence of SIRS development, sepsis, and the onset of sepsis and septic shock are shown in the investigated patient sample

* ANOVA

‡Kruskal–Wallis

Significant if P < 0.05

Binary logistic regression revealed the application of colloids to be an independent factor in the development of SIRS (Wald: 174.229; OR 3.325; P < 0.001) and sepsis (Wald: 108.989; OR 8.984; P < 0.001). However, EC, TC, and FFP revealed SIRS and sepsis to be an independent predictors for multiply injured patients (Table 3A). Interestingly, the onset was earliest in patients from the group receiving colloids <5L/48 h. ROC analysis showed the highest predictive power for SIRS (AUC 0.69; P < 0.001, CI 95 %, 0.653, 0.733; OR 3.33), followed by sepsis (AUC 0.669; P < 0.001; CI 95 %, 0.637, 0.706; OR 2.72) (Table 3B.).

Table 3

(A) The binary logistic regression analysis of the patient sample revealed that the infusion of colloids within the first 48 h after trauma is an independent predictor for the development of SIRS and sepsis. Hosmer–Lemeshow test, P < 0.001 for SIRS and P < 0.001 for sepsis. (B) ROC curve of the patient sample

Analysis of co-founding factors of SIRS and sepsis

The analysis revealed that in both groups, SIRS and sepsis, the GCS, base excess, and lactate played a significant permissive role for the development of SISR and sepsis in multiply injured patients (Table 5). The AIS spine, extremities, and pelvis as well as the prothrombin time, leukocyte counts, and APACHE II score had a significant effect on the development of SIRS and sepsis (Table 5.).

There is no doubt that polymeric saccharides such as HES can effectively expand blood volume and improve survival in patients with multiple injuries. The analysis submitted to the US Food and Drug Authority in the early 1970s would not be considered adequate to detect the possible side effects of HES in the present day. Since then, an increasing number of publications with concerns about HES, but with only partially selective outcome reporting (only positive outcomes) have been published [16–19]. In this retrospective cohort study, the focus was set on the application of polymeric plasma substitutes in the context of severe injury. Therefore, the question was asked how these substances influence the immunity system in multiple trauma patients. Patients who received more polymeric plasma substitute suffered significantly more severe SIRS and sepsis. Certainly, there are a lot of confounders for the development of SIRS and sepsis in multiply injured patients, but one key factor is the use of polymeric plasma substitutes, as supported by the highly significant binary logistic regression analysis (Table 3). Therefore, in this study, it may be concluded that besides other factors, polymeric plasma substitutes contribute significantly to the development of SIRS in multiply injured patients. However, the impact of injury severity on the development of SIRS and sepsis also plays a pivotal role [3]. Overactivation of the immune cells for the clearance of destroyed tissue might be the reason. The products used in this study vary over almost two decades; however, the one thing they all have in common is that they are all polymers. Polymeric substances might have pharmacologic effects on the reticulo-endothelial system (RES). There is growing evidence that polymeric plasma substitutes may inhibit the RES by inhibition of cytokine secretion [20]. The question of whether polymeric plasma expanders influence the RES was asked in the late 1980s. The application of HES reduced the phagocytic activity of RES; however, the data were unclear and lacked robust statistical analysis [21, 22]. Therefore, a partial immunosuppressive effect for polymeric plasma substitutes must be postulated. This seems to be reflected in the ORs obtained by the binary logistic regression, 3.325 for SIRS and 8.984 for sepsis (Table 3). Certainly, a higher trauma load in the patient sample receiving more polymeric plasma substitutes is obtained; therefore the trauma load and other factors also contribute to the development of SIRS and sepsis [3], which is indirectly reflected by the small AUC. How brain injury is involved in both SIRS and sepsis development remains speculative. The impaired blood–brain barrier under trauma conditions may release microglial cytokines to influence the immune system systemically. At this time, little is known about the influence of sugar polymers on immune physiology in humans; however, these data show that indications for their use in patients with multiple traumas should be clarified. The mixed outcomes might also be partly caused by the higher ISS at admission, but the polymeric plasma substitutes also seem to have a significant influence on pulmonary function in multiple trauma patients, as reflected by the ventilator-associated days in the ICU, the hospitalization duration, and the time of death, somehow in a paradox manner (Table 4). Interestingly, in this patient sample, the mortality was significantly lower in the group receiving colloids >5L/48 h. The ISS, APACHE II, and all other parameters except for age were significantly higher at admission for this patient group. Age was <40 years (37.4 ± 16.3 [a]). Whether such a significant break point for multiply injured patients occurs at about the age of 40 years remains speculative; however, age appears to play a pivotal role in the pathophysiology of multiply injured patients.

A limitation, and a possible source of bias, is the changing fluid resuscitation protocols over the study period, which could make the interpretation less reliable. The chosen selection criteria might counteract this bias.

Polymeric plasma substitutes should be applied to multiply injured patients in a more tailored fashion, because besides many other factors these plasma substitutes might permissively affect SIRS and sepsis. However, patient survival might be positively influenced by the application of polymeric plasma substitutes, as depicted in this sample.

Authors’ contributions

All authors contributed equally to this work. All authors read and approved the final manuscript.

Competing interests

The authors declare that they have no competing interests.

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American College of Chest Physicians/Society of Critical Care. Medicine consensus conference: definitions for sepsis and organ failure and guidelines for the use of innovative therapies in sepsis. Crit Care Med. 1992;20:864–74.View ArticleGoogle Scholar